Sequential therapy with recombinant interferons gamma and alpha in patients with unfavorable prognosis of chronic myelocytic leukemia: Clinical responsiveness to recombinant ifn‐α correlates with the degree of receptor down‐regulation

Bartsch, H. H.; Pfizenmaier, Klaus; Hanusch, A; Scheurich, Peter; Üçer, U.; Nagel, G. A.

doi:10.1002/ijc.2910430211

Cited by 14 publications

(6 citation statements)

References 36 publications

(42 reference statements)

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“…Pretreatment with LPS (0.1 #g/ml) also blocked MAP kinase activation induced by both stimuli but was only effective in C3H/HeN macrophages ( Table 1). Downregulation of kinase activation has been attributed to depletion of receptors by ligand binding (25,26). However, if LPS and LPP shared a receptor, then pretreatment with LPS should have contributed to the reduction of MAP kinase activation in C3H/HeJ macrophages.…”

Section: Resultsmentioning

confidence: 99%

Tyrosine phosphorylation of mitogen-activated protein kinases is necessary for activation of murine macrophages by natural and synthetic bacterial products.

Dong

Fidler

1993

The Journal of Experimental Medicine

126

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SummaryThe purpose of these studies was to determine the intracellular signal transduction pathways of bacterial products in murine macrophages from lipopolysaccharide (LPS)-responder C3H/HeN and LPS-nonresponder C3H/HeJ mice. Both LPS and synthetic lipopeptide CGP 31362 (LPP) induced production of tumor necrosis factor c~ (TNF-oe) in C3H/HeN macrophages. In C3H/HeJ macrophages, however, TNF-oe was induced only by incubation with LPP. Both LPS and LPP induced tyrosine phosphorylation on proteins with apparent molecular masses of 39, 41, and 45 kD (p35, p41, and p45) in C3H/HeN macrophages, whereas in C3H/HeJ macrophages, tyrosine phosphorylation was induced only by LPP. 20-h incubation with LPS or LPP downregulated TNF-oL production/secretion and tyrosine phosphorylation in C3H/HeN macrophages induced by additional LPS or LPP. In C3H/HeJ macrophages, however, the downregulation of TNF-a production and tyrosine phosphorylation were observed only with LPP. Protein kinase assays, Western blotting analyses, phenyl-Sepharose chromatography, and immunocomplex kinase assay suggested that p45 and p39 were similar or identical to mitogenactivated protein (MAP) kinase 1 and 2, respectively. Pretreatment of macrophages with LPS or LPP did not change the amount of kinase proteins but inhibited the stimulation of kinase activity by the agents. These data suggest that MAP kinases are among target proteins involved in the transduction of LPS and LPP signals that lead to activation of murine macrophages to produce/secrete TNF.

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Section: Resultsmentioning

confidence: 99%

Tyrosine phosphorylation of mitogen-activated protein kinases is necessary for activation of murine macrophages by natural and synthetic bacterial products.

Dong

Fidler

1993

The Journal of Experimental Medicine

126

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“…So far, this type of regulation has been described for a number of receptors for growth factors and cytokines. For example, IFN-u receptors, which have been extensively studied, were found to be downregulated after treatment with IFN-a in all the cell types tested both in vitro and in vivo [19] .This down-regulation is considered as a marker of the action of IFN-a and correlates with the clinical responses of patients with B cell malignancies such as hairy cell leukemia and non-Hodgkin's lymphoma [16,20,211 and also with chronic myeloid leukemia [22] , i. e. tumors which are particularly sensitive to IFN-a therapy [23]. By contrast, down-regulation of insulin receptors seems to correlate with insulin resistance in some forms of type I1 diabetes [24].…”

Section: Discussionmentioning

confidence: 99%

Differential regulation of interleukin‐6 receptors by interleukin‐6 and interferons in multiple myeloma cell lines

Lasfar

Billard

1994

Eur J Immunol

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Interleukin-6 (IL-6) mediates pleiotropic functions through specific receptors (IL-6R) composed of an 80-kDa binding protein, associated with a non-ligand binding protein (gp130) which transduces the signal. Because IL-6 is the major tumor growth factor in multiple myeloma, we investigated the regulation of IL-6R in two human multiple myeloma cell lines. Binding experiments with 125I-labeled IL-6 showed that IL-6R were expressed at a high density on RPMI-8226 cells (15 000 receptors/cell), but no specific binding was detected on XG-1 cells, whose growth depends on the presence of exogenous IL-6. However, when IL-6 was removed from the culture medium, high-affinity IL-6R appeared on the surface of XG-1 cells (5300 sites/cell). Treatment of RPMI-8226 cells with IL-6 reduced the number of IL-6R without changing their affinity. This reduction was dose dependent and was not affected by acid treatment which dissociates ligand-receptor complexes. Cross-linking experiments showed that the formation of one IL-6/receptor complex of 160 kDa markedly decreased upon IL-6 treatment, while the other complex of 190 kDa became undetectable. These data provide evidence for ligand-induced down-regulation of membrane IL-6R expression in myeloma cells. Treatment of RPMI-8226 cells with interferon-alpha (IFN-alpha), which inhibits the growth of these cells, stimulated IL-6R expression and increased the formation of the 160-kDa IL-6/receptor complex. This stimulation was specific for IFN-alpha, since IFN-gamma reduced the number of IL-6R. These data indicate that, in myeloma cells, IL-6R are differentially regulated by IL-6 and IFN-alpha.

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“…In good responders, a permanent ‘down‐regulated’ state of IFNAR2 was maintained at least for 12 months after the initiation of the IFN α therapy, indicating that long‐term down‐regulation of IFN receptor seems to reflect a continuous response to IFN α . Earlier studies, which were performed by receptor‐binding assays because IFN receptor subunits had not been identified yet, reported the modulations of type I IFN receptor on PBMNCs during IFN α therapy in CML patients (31–33), where the decrease of ligand‐receptor binding occurred in patients achieving a good response but not in patients with a poor response to IFN α . One of these studies also reported that the down‐regulation of the IFN receptor occurred even with in vitro treatment of IFN α , and that this decreased binding was due to a loss in number of IFN receptors, not due to decrease of affinity to the ligand (31).…”

Section: Discussionmentioning

confidence: 99%

“…It has been investigated whether IFN receptor expression and its down‐regulation are related to the clinical response to IFN α in hematological malignancies such as hairy cell leukemia (29), low‐grade malignant lymphoma (30), and CML. Comprehensive studies on IFN receptor expressions in relation to the clinical response to IFN α therapy in CML have been rather limited, except in earlier studies by receptor‐binding assays (31–33). Even after molecular cloning of the IFNAR1 and IFNAR2, studies regarding the IFN receptor expression in clinical samples of hematological malignancies have been very limited.…”

mentioning

confidence: 99%

“…Moreover, it is reported that IFN receptor expression on CD34‐positive cells increases with cell differentiation (36, 37). In this context, in order to precisely clarify the IFN α action in CML patients, it is important to focus on CD34‐positive cells, but not on PBMNCs or bone marrow mononuclear cells (BMMNCs) as all other previous studies reported (31–34).…”

mentioning

confidence: 99%

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Initial expression of interferon alpha receptor 2 (IFNAR2) on CD34‐positive cells and its down‐regulation correlate with clinical response to interferon therapy in chronic myelogenous leukemia

Ito

Tanaka

Ito

et al. 2004

European J of Haematology

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In order to investigate the mechanism of interferon-alpha (IFNalpha) action in the treatment of chronic myelogenous leukemia (CML), we examined surface expressions of both type I interferon receptor 1 (IFNAR1) and 2 (IFNAR2) subunits on CD34-positive cells in bone marrow (BM) in a total of 57 CML patients. Initial cell-surface IFNAR2 expression at diagnosis assessed by flow cytometry widely distributed but showed overall significantly higher expression in CML patients when compared with normal controls. In 15 fresh patients who subsequently received IFNalpha therapy, IFNAR2 expression at diagnosis was significantly higher in cytogenetic good responders than in poor responders. Down-regulation of IFNAR2 expression during IFNalpha therapy was observed only in good responders but not in poor responders. In addition to protein level, both initial high IFNAR2c mRNA expression level and its down-regulation during IFNalpha therapy, in purified CD34-positive cells, were also observed only in good responders. In contrast to IFNAR2, cell-surface IFNAR1 expression was generally lower than IFNAR2, and correlation between either the pretreatment level or down-regulation of IFNAR1 and clinical response was not evident. With in vitro IFNalpha stimulation, CD34-positive cells showed down-regulations of cell-surface IFNAR2, and IFNAR1 to a lesser extent, in one good-responder patient, but not in one poor-responder patient. Serum soluble interferon receptor (sIFNR) was higher in untreated CML patients than in normal controls, without any correlation with clinical response to IFNalpha. Thus, the pretreatment protein and mRNA expression levels of IFNAR2 and their down-regulations during IFNalpha therapy correlate well with IFNalpha response in CML patients.

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Sequential therapy with recombinant interferons gamma and alpha in patients with unfavorable prognosis of chronic myelocytic leukemia: Clinical responsiveness to recombinant ifn‐α correlates with the degree of receptor down‐regulation

Cited by 14 publications

References 36 publications

Tyrosine phosphorylation of mitogen-activated protein kinases is necessary for activation of murine macrophages by natural and synthetic bacterial products.

Tyrosine phosphorylation of mitogen-activated protein kinases is necessary for activation of murine macrophages by natural and synthetic bacterial products.

Differential regulation of interleukin‐6 receptors by interleukin‐6 and interferons in multiple myeloma cell lines

Initial expression of interferon alpha receptor 2 (IFNAR2) on CD34‐positive cells and its down‐regulation correlate with clinical response to interferon therapy in chronic myelogenous leukemia

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